Rizan Nashef scite author profile

Background: Bacteria evade host defense peptides by degradation. Results: Actin protects the LL-37 antimicrobial peptide and enables its bactericidal action in the presence of bacterial proteases. Conclusion: Sites of infection and necrosis are likely to contain high amounts of actin that will protect LL-37 from degradation. Significance: Components released from lysed cells can be used to enhance local immunity.

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Oral fibroblasts modulate the macrophage response to bacterial challenge

Tzach-Nahman

Nashef

Fleissig

et al. 2017

Sci Rep

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Tissue damage in chronic periodontal disease is driven by the host response to a dysbiotic microbiota, and not by bacteria directly. Among chronic inflammatory diseases of the oral cavity, inflammation and tissue damage around dental implants (peri-implantitis) is emerging as a major clinical challenge, since it is more severe and less responsive to treatment compared to inflammation around natural teeth. We tested whether oral fibroblasts from the periodontal ligament (PDLF), which are present around natural teeth but not around dental implants, actively regulate inflammatory responses to bacterial stimulation. We show that human PDLF down-regulate TNF-α post-transcriptionally in macrophages stimulated with the oral pathogen Porphyromonas gingivalis. Cell contact and secretion of IL-6 and IL-10 contribute to the modulation of inflammatory cytokine production. Although fibroblasts decreased TNF-α secretion, they enhanced the ability of macrophages to phagocytose bacteria. Surprisingly, donor matched oral fibroblasts from gingival tissues, or fibroblasts from peri-implant inflamed tissues were at least as active as PDLF in regulating macrophage responses to bacteria. In addition, priming fibroblasts with inflammatory mediators enhanced PDLF regulatory activity. A further understanding of the spectrum of fibroblast activities in inflammatory lesions is important in order to design ways to control inflammatory tissue damage.

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Rizan Nashef

Actin Enables the Antimicrobial Action of LL-37 Peptide in the Presence of Microbial Proteases

Oral fibroblasts modulate the macrophage response to bacterial challenge

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